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Design, crystal structure and atomic force microscopy study of thioether ligated D, L-cyclic antimicrobial peptides against multidrug resistant Pseudomonas aeruginosa

机译:硫醚连接的D,L-循环抗微生物肽对多药抗性铜绿假单胞菌的设计,晶体结构和原子力显微镜研究

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摘要

Here we report a new family of cyclic antimicrobial peptides (CAMPs) targeting MDR strains of Pseudomonas aeruginosa. These CAMPs are cyclized via a xylene double thioether bridge connecting two cysteines placed at the ends of a linear amphiphilic alternating D, L-sequence composed of lysines and tryptophans. Investigations by transmission electron microscopy (TEM), dynamic light scattering and atomic force microscopy (AFM) suggest that these peptide macrocycles interact with the membrane to form lipid-peptide aggregates. Amphiphilic conformations compatible with membrane disruption are observed in high resolution X-ray crystal structures of fucosylated derivatives in complex with lectin LecB. The potential for optimization is highlighted by N-methylation of backbone amides leading to derivatives with similar antimicrobial activity but lower hemolysis.
机译:在这里,我们报告了靶向铜绿假单胞菌的MDR菌株的新循环抗菌肽(阵营)。 这些阵营通过连接到由赖氨酸和色氨酸组成的线性两亲交替的D,L序列的末端的二甲苯双硫醚桥来通过二甲苯双硫醚桥来环化。 通过透射电子显微镜(TEM),动态光散射和原子力显微镜(AFM)的研究表明,这些肽宏杂种与膜相互作用以形成脂质肽聚集体。 在与凝集素LECB的岩藻糖苷化衍生物的高分辨率X射线晶体结构中观察到与膜破坏相容的两亲构象。 通过骨架酰胺的N-甲基化导致具有相似抗微生物活性但溶血性较低的衍生物的N-甲基化突出显示。

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  • 来源
    《Chemical science》 |2017年第11期|共12页
  • 作者单位

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Geneva Univ Hosp Geneva Serv Infect Dis Dept Microbiol &

    Mol Med Geneva Switzerland;

    Univ Geneva Univ Hosp Geneva Serv Infect Dis Dept Microbiol &

    Mol Med Geneva Switzerland;

    Univ Geneva Univ Hosp Geneva Serv Infect Dis Dept Microbiol &

    Mol Med Geneva Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

    Univ Bern Dept Chem &

    Biochem Freiestr 3 CH-3012 Bern Switzerland;

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  • 正文语种 eng
  • 中图分类 化学;
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